Topics in Oncology

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Topics in Oncology

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Title: Topics in Oncology

1
Topics in Oncology

New Advances in Targeted Therapy for Colorectal
Cancer

2
Program Overview

Incidence and epidemiology
Diagnosis and screening
Metastatic CRC
Chemotherapy
Targeted therapy
Antiangiogenesis
EGFR-targeted therapy
New directions for targeted therapy
Adjuvant CRC
Improving outcomes in colorectal cancer
Quality of care
Patient management
Other GI cancers

3
CRC Incidence and Epidemiology
4
2006 Estimated New Cancer Cases in US
Leading Sites by Sex

Men
Prostate 33
Lung and bronchus 13
Colon and rectum 10
Urinary bladder 6

Women 31 Breast 12 Lung and bronchus 11 Colon
and rectum 6 Uterine corpus
gt55,000 Total Colorectal Cancer Deaths
Image adapted from http//caonline.amcancersoc.or
g/cgi/content/full/55/1/10 American Cancer
Society. Cancer Facts and Figures 2006. Atlanta
ACS 2006.
5
Colorectal Cancer

Second leading cause of cancer-related death in
the US
145,000 new cases diagnosed each year in the US
75 of new cases in patients with no family
history of CRC or predisposing illness
Between 1995-2000, 20 of patients presented with
metastatic disease at initial diagnosis

American Cancer Society. Colorectal Cancer Facts
Figures Special Edition 2005. 2005 1-24.
6
Gastrointestinal Cancers in the United States
Other digestive organs
Small intestine2
Anus
2
2
Gallbladder
3
Esophagus
6
Liver
7
Colon
41
Stomach
8
Pancreas
13
Rectum
16
American Cancer Society. Cancer Facts and Figures
2006. Atlanta American Cancer Society 2006.
7
Screening for Colorectal Cancer

Screening methods
Fecal occult blood testing
Colonoscopy
Sigmoidoscopy
Double-contrast barium enema
NCCN recommendation for average-risk persons
FOBT and flexible sigmoidoscopy every 5 years or
Colonoscopy every 10 years

NCCN Guidelines. Version 2.2006 April 2006.
8
Risk Factors for Colorectal Cancer

CRC in first-degree family member or in 2
second-degree
Genetic1
Familial adenomatous polyposis (FAP)
Hereditary nonpolyposis colorectal cancer (HNPCC)
Nongenetic1
History of adenomas
Endometrial or ovarian cancer before age 60
Inflammatory bowel disease
Lifestyle factors possibly associated with
increased risk2
Western diet, sedentary lifestyle, alcohol,
smoking

1. NCCN Guidelines. Version 2.2006 April
2006. 2. Ahmed FE. J Environ Sci Health C Environ
Carcinog Ecotoxicol Rev. 20042291-147.
9
Staging of Colorectal Cancer
NCCN Guidelines. Version 2.2006 April 2006.
10
Lymph Node Evaluation in CRC

Minimum of 12 LN suggested to identify stage II
CRC according to AJCC, CAP
Controversy surrounds number of LN needed
Factors affecting number of LN retrieved
Age
Gender
Tumor grade
Tumor site

NCCN Guidelines. Version 2.2006 April 2006.
11
Disease Stage at Initial Diagnosis of Colon
Cancer
5
Localized
19
Regional
Distant
39
Unstaged
38
SEER Program (www.seer.cancer.gov) SEERStat
Database Incidence. Released April 2005.
12
Disease-free Survival in Patients with Colon
Cancer
13
Prognostic Factors in CRC

Poor prognostic factors
Bowel obstruction, perforation1
Factors determined retrospectively, not
prospectively validated
Thymidylate synthase2
18q deletion3
Number LN examined in colon, rectal surgery4
Microsatellite instability
Improved survival in younger patients5

1. Steinberg M, et al. Cancer. 1986571866-1870
2. Johnston PG, et al. J Clin Oncol.
1994122640-2647 3. Jen J, et al. N Engl J Med.
1994331213-221 4. Le Voyer TE, et al. J Clin
Oncol. 2003212912-2919 5. Gryfe R, et al. N
Engl J Med. 200034269-77.
14
Surgical Approaches in the Treatment of
Colorectal Cancer

Surgery for resectable colon cancer
Colectomy with en bloc removal of regional LN
Laparoscopic-assisted surgery may be feasible
Surgery for rectal cancer
Transabdominal resection or transanal excision
for certain patients with T1, T2 lesions
Abdominal peritoneal resection or low anterior
resection with TME for all others
Preoperative or postoperative chemoradiotherapy
for serosal invasion/regional node involvement

1. Clinical Outcomes of Surgical Therapy Study
Group. N Engl J Med. 20043502050-2059. 2. NCCN
Guidelines. Version 2.2006 November 2005.
15
Metastatic Colorectal Cancer
16
Treatment for Metastatic CRC

Bolus FU/LV standard of care in US until 2000
Five agents approved by FDA for mCRC since 1998
Irinotecan
Oxaliplatin
Capecitabine
Bevacizumab
Cetuximab
Median overall survival extended with newer agents

Venook A. Oncologist. 200510250-261.
17
NCCN-recommended Regimens for Metastatic CRC
Venook A. Oncologist. 200510250-261.
18
N9741 IFL vs FOLFOX vs IROX
RANDOMIZE
Irinotecan and bolus 5-FU leucovorin (IFL) (n26
4)

N792
Previously untreated mCRC

Oxaliplatin, infused 5-FU leucovorin (FOLFOX) (n
267)
Irinotecan and oxaliplatin (IROX) (n264)
Goldberg RM, et al. J Clin Oncol. 20042223-30.
19
N9741 FOLFOX Increases Overall Survival
Goldberg RM, et al. J Clin Oncol. 20042223-30.
20
N9741 Less Overall Toxicity with FOLFOX vs IFL

Less diarrhea, vomiting, nausea, febrile
neutropenia, dehydration with FOLFOX vs IFL1
More paresthesias, neutropenia with FOLFOX
More patients discontinued FOLFOX due to toxicity
than progression
Caucasians (n1297) vs African Americans (n112)2
Higher ORR in Caucasians (OR 1.72 P0.012)
Lower toxicity in AA
Primarily less diarrhea
OR for severe toxicity in Caucasians, 1.76
(P0.006)

1. Goldberg RM, et al. J Clin Oncol.
20042223-30. 2. Goldberg RM, et al. ASCO 2006.
Abstract 3503.
21
N9741 IFL vs FOLFOX vs IROX

In first-line mCRC, survival longer with FOLFOX
vs
IFL (irinotecan and bolus 5-FU leucovorin) or
IROX (irinotecan and oxaliplatin)
Median OS
19.5 mo, 15.0 mo, 17.4 mo
Most grade 3/4 adverse events less common with
FOLFOX
Only paresthesias, neutropenia more common

Goldberg RM, et al. J Clin Oncol. 20042223-30.
22
FOLFOX4 Maintains Efficacy/ Safety Ratio in
Elderly Patients

Retrospective analysis of patients receiving
FOLFOX4
3,742 patients 614 aged gt70 years
Grade 3/4 AEs more frequent in older patients
Neutropenia (43 vs 49 P0.04)
Thrombocytopenia (2 vs 5 P0.04)
No difference in 60-day mortality
No difference in FOLFOX4 efficacy

Goldberg RM, et al. 2006 ASCO GI. Abstract 228.
23
FOLFIRI Equivalent to FOLFOX4

Phase III randomized trial compared FOLFIRI to
FOLFOX4 in first-line advanced CRC
Survival, response rates similar between groups
Toxicity mild but differed by treatment
FOLFOX
Thrombocytopenia
Neurosensory toxicities
FOLFIRI
Alopecia
GI disturbances

Colucci G, et al. J Clin Oncol. 2005234866-4875.
24
UGT1A1 and Irinotecan Toxicity

Individuals homozygous for UGT1A128 allele at
increased risk of neutropenia
Gilberts syndrome
Allele detectable by molecular assay (Invader
UGT1A1 Molecular Assay)
Consider reduced initial irinotecan dose for
these patients

Camptosar (irinotecan HCL injection) Prescribing
Information. New York, NY Pfizer, Inc. July
2005 Invader UGT1A1 Molecular Assay Product
Information. Madison, WI Third Wave
Technologies, Inc. August 12, 2005.
25
Phase III GERCOR Study FOLFOX6/FOLFIRI Sequence
RANDOMIZE
Folinic acid, FU, irinotecan (FOLFIRI) (n109)
Folinic acid, FU, oxaliplatin (FOLFOX6) (n81)

N220
Previously untreated mCRC

Folinic acid, FU, oxaliplatin (FOLFOX6) (n111)
Folinic acid, FU, irinotecan (FOLFIRI) (n69)
Tournigand C, et al. J Clin Oncol.
200422229-237.
26
FOLFOX6/FOLFIRI Sequences Equivalent

FOLFIRI more grade 3/4 mucositis, grade 2
alopecia
FOLFOX6 more grade 3/4 neutropenia, neurosensory
toxicity

In first-line In second-line. Tournigand C,
et al. J Clin Oncol. 200422239-237.
27
Importance of Individualizing Treatment Approach

Optimal sequence of chemotherapy regimens unknown
Important to consider patient factors
Tolerability for different toxicities
More bowel dysfunction ? may prefer oxaliplatin
Performance status
Patient wishes

28
FOLFOXIRI vs FOLFIRI
RANDOMIZE
FOLFIRI Irinotecan (180 mg/m2 d1) I-LV (100
mg/m2 d1,2) bolus 5FU (400 mg/m2 d1,2) 5FU
(600 mg/m2 22 h inf on d1,2) (n122)
N244 Previously untreated mCRC
Repeat q2 wk until progression
Repeat q2 wk until progression
FOLFOXIRI Irinotecan (165 mg/m2 d1) Oxaliplatin
(85 mg/m2 d1) I-LV (200 mg/m2 d1) 5FU (3200
mg/m2 48 h inf starting on d1) (n122)
Falcone A, et al. ASCO GI 2006. Abstract 227.
29
FOLFOXIRI More Effective Than FOLFIRI

Overall response rate significantly higher with
FOLFOXIRI
66 vs 41 with FOLFIRI (P0.0002)
At median FU of 14.0 months, PFS longer with
FOLFOXIRI
Median PFS, 9.8 vs 6.8 months P0.0003)
FOLFOXIRI associated with significantly more
grade 2/3 neurotoxicity (20 vs 0 Plt0.0001)

Falcone A, et al. ASCO GI 2006. Abstract 227.
30
Survival Correlates with Availability of All
Effective Drugs
3 drugs 5-FU/LV, irinotecan, oxaliplatin. Grothey
A, et al. J Clin Oncol. 2005239441-9442.
31
Targeted Therapies in Metastatic Colorectal Cancer
32
Introduction to Targeted Therapy

Agent targets specific pathway in the
growth/development of malignant cells
Current types of biologic therapy
Tyrosine kinase receptor inhibitors
Antibodies, small molecule inhibitors
Angiogenesis inhibitors
Proteasome inhibitors
Immunotherapy
Others

33
VEGF Primary Mediator of Angiogenesis

Promotes endothelial cell viability and
proliferation
Chemotaxis
Increases expression of collagenase, tPA, and uPA
Increases vascular permeability and vasodilation
Inhibits maturation of antigen-presenting
dendritic cells

tPA, tissue plasminogen activator uPA, urokinase
plasminogen activator.
34
VEGF Family and Its Receptors
VEGF-A
VEGF-B
VEGF-C
VEGF-D
PIGF
0
0
0
0
0
VEGFR-2 (Flk-1/KDR)
NRP-1 (Neuropilin)
VEGFR-3 (Flt-4)
VEGFR-1 (Flt-1)
Unclear, but likely involved in tumor
growth (non-RTK)
Angiogenesis, lymphangiogenesis (RTK)
Angiogenesis (RTK)
Lymphangiogenesis (RTK)
RTK, receptor tyrosine kinase. Dvorak HF. J Clin
Oncol. 2002204368 Ferrara N, et al. Nat Med.
20039669.
35
Inhibition of VEGF

Inhibits metastasis
Blocks VEGF-induced peritumor lymph drainage1
Blocks VEGF(A)-induced dysfunctional
angiogenesis2
Inhibits invasion of circulation by the tumor3
Decreases vascular density of tumor
Increases killing of established tumors
Improves chemotherapy delivery to tumor

1. Dafni H, et al. Cancer Res. 2002626731-6739.
2. Nagy JA, et al. J Exp Med. 20021961497-1506.
3. Weis S, et al. J Cell Biol. 2004167223-229.
36
Mechanisms of Inhibiting VEGF
Ligand sequestration mAbs, soluble
receptors (eg, bevacizumab)
VEGF
Tyrosine kinase inhibition TKIs (eg, SU11248)
Receptor-blockingmAbs (eg, IMC-1121)
p85
VEGFR
ras
GRB2
SOS
PLCg
Transcription factor inhibition
36
37
Phase III Trial Bevacizumab IFL
RANDOMIZE
Irinotecan, bolus FU, leucovorin (IFL) 5 mg/kg
bevacizumab q2 wk (n402)
N813 Previously untreated mCRC
Stratified by study center, ECOG PS, colon vs
rectal disease, no. metastatic sites
Irinotecan, bolus FU, leucovorin (IFL)
Placebo (n411)
Hurwitz H, et al. N Engl J Med.
20043502335-2342.
38
Survival Benefit When Bevacizumab Added to IFL
Hurwitz H, et al. N Engl J Med.
20043502335-2342.
39
Bevacizumab IFL Safety
Hurwitz H, et al. N Engl J Med.
20043502335-2342.
40
Bevacizumab Safety Issues Thromboembolic Events

Potential events
Stroke, MI, TIA, angina, other arterial
thromboembolic events
Older patients at particular increased risk
Age gt65 years
8.5 vs 2.9 on chemotherapy alone
Age lt65 years
2.1 vs 1.4
Permanently discontinue bevacizumab in patients
who develop severe arterial thromboembolic event
during treatment

Avastin (bevacizumab) Prescribing Information.
So. San Francisco, CA Genentech, Inc. February
2004.
41
Bevacizumab Safety Issues GI Perforation

GI perforation, wound dehiscence can result in
death
GI perforation occurred in 2 of patients
receiving bevacizumab plus bolus IFL
Typical presentation
Abdominal pain with constipation/vomiting
Discontinue bevacizumab permanently if bowel
perforation or wound dehiscence requiring medical
intervention
Proper interval between bevacizumab treatment and
surgery occurs is unknown

Avastin (bevacizumab) Prescribing Information.
So. San Francisco, CA Genentech, Inc. February
2004.
42
Bevacizumab Safety Issues Hypertension

1.7 of patients developed HT resulting in
hospitalization or treatment discontinuation
Temporarily stop BEV if uncontrolled severe HT
develops
Permanently discontinue BEV if hypertensive
crisis develops
Monitor BP at least every 2 to 3 weeks
More frequently in those who develop hypertension

Across all clinical studies (N1032). Avastin
(bevacizumab) Prescribing Information. So. San
Francisco, CA Genentech, Inc. February 2004.
43
Bevacizumab Safety Issues Hemorrhage

Bevacizumab linked to infrequent cases of
hemoptysis, GI hemorrhage, subarachnoid
hemorrhage, and hemorrhagic stroke
Grade 1 epistaxis occurred in 35 of patients
receiving BEV IFL
Generally mild and resolved spontaneously
CNS bleeding risk in patients with CNS metastases
unknown
Patients with serious hemorrhage should
discontinue BEV
Those with recent hemoptysis should not receive
BEV

Avastin (bevacizumab) Prescribing Information.
So. San Francisco, CA Genentech, Inc. February
2004.
44
E3200 High-dose BEV FOLFOX4 Study Design
FOLFOX4 Bevacizumab (BEV 10 mg/kg q2 wk)
(n289)
RANDOMIZE
N822 Previously treated mCRC
FOLFOX4 (n290)
Bevacizumab (10 mg/kg q2 wk) (n243)
Stratified by study center, ECOG PS, prior XRT
Giantonio BJ, et al. ASCO 2005. Abstract 2.
45
Improved Survival with High-dose Bevacizumab
FOLFOX4
P-value compares BEV FOLFOX4 vs
FOLFOX4. Giantonio BJ, et al. ASCO 2005.
Abstract 2.
46
E3200 High-dose Bevacizumab FOLFOX4 Safety

Grade 3/4 AEs significantly more frequent with
adding bevacizumab
Hypertension
Bleeding
Neuropathy
Vomiting
Grade 3/4 arterial, venous thromboses equivalent
Bowel perforation occurred in 1 of BEV-treated
patients

Giantonio BJ, et al. ASCO 2005. Abstract 2.
47
Benefit of Adding Bevacizumab to FOLFOX4

Adding bevacizumab to FOLFOX4 lengthened overall
survival by 24
Hypertension, bleeding, vomiting more common with
bevacizumab FOLFOX4
Bowel perforation occurred at rate of 1 with
bevacizumab
Bevacizumab not active as single agent

Giantonio BJ, et al. ASCO 2005. Abstract 2.
48
TREE-1/2 Bevacizumab Oxaliplatin
Fluoropyrimidine
mFOLFOX6 BEV q2 wk Bevacizumab (5 mg/kg d1)
Oxaliplatin (85 mg/m2) LV (fixed dose 350
mg) 5-FU (400 mg/m2 IV bolus followed by 2400
mg/m2 IV inf over 46 h d1) (n71)
RANDOMIZE

N213
Previously untreated mCRC
Unresectable
Adequate organ function

bFOL BEV q28 d Bevacizumab (5 mg/kg d1,
15) Oxaliplatin (85 mg/m2 d1, 15) LV (20 mg/m2
IV bolus d1, 8, 15) 5-FU (500 mg/m2 IV bolus d1,
8, 15) (n71)
CapeOx BEV q21 d Bevacizumab (7.5 mg/kg
d1) Oxaliplatin (130 mg/m2 d1) Capecitabine (850
mg/m2 bid d1-15 d1 PM only, d15 AM only) (n71)
Hochster H, et al. ASCO 2006. Abstract 3510.
49
Addition of Bevacizumab Improves Efficacy of All
Three Regimens
TTP, time from randomization to objective tumor
progression or death. Hochster H, et al. ASCO
2006. Abstract 3510.
50
TREE-2 Conclusions

No significant additive toxicities when
bevacizumab combined with any regimen
Bevacizumab improved RR, TTP, OS of all regimens
(over TREE-1 results)
CapeOx tolerability improved when CAPE dose
reduced to 850 mg/m2 bid

Hochster H, et al. ASCO 2006. Abstract 3510.
51
BRiTE Trial Bevacizumab Safety in Community
Setting

BRiTE Trial
Safety in 1968 patients taking BEV
12 had related SAEs after median 10 mo
Arterial thromboembolic events, 2.1
Grade 3/4 bleeding, 1.9
GI perforation, 1.7
Postop bleeding/wound healing complications, 1.2
New hypertension requiring medication, 8.9
Worse hypertension in patients already treated at
baseline, 6.2

Hedrick E, et al. ASCO 2006. Abstract 3536.
52
CONCEPT Continuous Oxaliplatin Neurotoxicity
Prevention Trial
RANDOMIZE
mFOLFOX7 bevacizumab (continuous) /- IV
Calcium/magnesium

Previously untreated mCRC
(initiated 2/05)

mFOLFOX7 bevacizumab (intermittent
oxaliplatin) /- IV Calcium/magnesium
Study Director, Gilbert Jirau-Lucca, MS,
Bridgewater, NJ Sanofi-Aventis.
53
OPTIMOX2 Maintenance vs Chemotherapy-free
intervals
RANDOMIZE
mFOLFOX7 No maintenance until baseline
progression mFOLFOX7 reintroduction (n102)
N202 Previously untreated mCRC
mFOLFOX7 sLV5FU2 until baseline
progression mFOLFOX7 reintroduction (n100)
Maindrault-Goebel F, et al. ASCO 2006. Abstract
3504.
54
Chemotherapy-free Intervals Feasible in Some
Patients after FOLFOX

Suggests break in therapy feasible in patients
responding to first- line FOLFOX

Maindrault-Goebel F, et al. ASCO 2006. Abstract
3504.
55
Bevacizumab Demonstrates Value of Targeted Therapy

Bevacizumab is the first targeted agent to show
survival benefit in metastatic CRC
Ongoing trials investigating optimal use of
bevacizumab
EGFR pathway represents another attractive target
Involved in tumor cell growth, resistance to
apoptosis, and metastasis

56
EGF-induced Signal Transduction and Tumorigenesis
EGF

EGFR
A large tyrosine kinase growth factor receptor
Natural ligands
TGF-?, EGF
Potential to block multiple steps in the signal
transduction process
Extracellular surface
Intracellular targets

()
EGFR
X
Anti-EGFR
K
K
PI3-K
pY
pY
MEK
pY
STAT
PTEN
AKT
MAPK
Gene transcription Cell-cycle progression
p27
X
X
X
X
Proliferation
Invasion/ metastasis
Survival/ anti-apoptosis
Angiogenesis
Perez-Soler R. Oncologist. 2004958-67.
57
Incidence of EGFR Expression in Solid Tumors
SCCHN, squamous cell carcinoma of the head and
neck. Arteaga C. Semin Oncol. 200330(suppl
7)3-14.
58
Anti-EGFR Strategies
Toxin conjugates
mAbs
TKIs
Ligand
Antisense
Cetuximab
Panitumumab
Ligand
Ligand
Ligand
mAb
Gefitinib Erlotinib
TKI
K
K
K
K
K
K
K
K
Survival and metastasis
Signal transduction
Protein synthesis
Cell death
Adapted from Raymond E, et al. Drugs.
200060(suppl 1)15-23.
59
Cetuximab Chimeric Anti-EGFR

Mousehuman chimeric mAb
Active alone or in combination with irinotecan in
irinotecan-refractory patients
Currently approved for patients with
irinotecan-refractory metastatic CRC

Cunningham D, et al. N Engl J Med.
2004351337-345. Shitara K, et al. Cancer
Immunol Immunother. 199336373-380.
60
BOND I Cetuximab /- Irinotecan
RANDOMIZE
Cetuximab irinotecan Cetuximab (initial dose,
400 mg/m2 then weekly infusion 250 mg/m2)
irinotecan (same as prestudy therapy) (n218)

N329
Patients with mCRC who progressed during or
within 3 mo after irinotecan

Cetuximab (initial dose, 400 mg/m2 then weekly
infusion 250 mg/m2) (n111)
Histamine receptor antagonist premedication given
before at least the first cetuximab infusion.
Cunningham D, et al. N Engl J Med.
2004351337-345.
61
Cetuximab Irinotecan Active in
Irinotecan-refractory Tumors
Cunningham D, et al. N Engl J Med.
2004351337-345.
62
EGFR Expression and Responses to Cetuximab

EGFR expression did not correlate with responses
to cetuximab

Cunningham D, et al. N Engl J Med.
2004351337-345.
63
Cetuximab Active in EGFR-negative CRC

16 irinotecan-refractory, EGFR-negative CRC
patients received cetuximab in nonstudy setting
at MSKCC
ORR, 25 (95 CI, 4-46)
Indicates EGFR analysis by currently available
IHC not predictive
Suggests against selecting, excluding patients
based on EGFR expression as measured by currently
available IHC

Chung KY, et al. J Clin Oncol. 2005231803-1810.
64
Predictive Value of EGFR Inhibitor-associated Rash

Rash associated with superior responses to
treatment
Indicates rash can be surrogate marker of
activity
Presence of any rash conferred significant
survival benefit (P0.02)
Trend toward improved survival with increasing
severity of rash
Cause of correlation currently unknown

Cunningham D, et al. N Engl J Med.
2004351337-345.
65
EGFR Inhibitor-associated Rash
Acneform rash on face
Paronychial inflammation
Acneform rash on chest
Segaert S, Van Cutsem E. Ann Oncol.
2005161425-1433.
66
BOND II Bevacizumab Cetuximab /- Irinotecan
Bevacizumab Cetuximab Bevacizumab (5 mg/kg q2
wk) Cetuximab (400 mg/m2 initial dose then 250
mg/m2 weekly) (n40)
RANDOMIZE

N81
Patients with CRC who progressed on irinotecan
EGFR expression not required
No prior bevacizumab or cetuximab

Bevacizumab Cetuximab Irinotecan Bevacizumab
(5 mg/kg q2 wk) Cetuximab (400 mg/m2 initial dose
then 250 mg/m2 weekly) Irinotecan (same dose as
prev therapy) (n41)
Saltz LB, et al. ASCO 2005. Abstract 3508.
67
BOND II Cetuximab/Bevacizumab /- Irinotecan
Efficacy
Saltz LB, et al. ASCO 2005. Abstract 3508.
68
BOND II Cetuximab/Bevacizumab /- Irinotecan
Safety
Saltz LB, et al. ASCO 2005. Abstract 3508.
69
CALGB 80203 FOLFIRI or FOLFOX Cetuximab in mCRC
FOLFIRI Cetuximab (n58)
RANDOMIZE

N224
Patients with previously untreated mCRC
Tissue available for EGFR testing

FOLFIRI (n55)
FOLFOX Cetuximab (n53)
FOLFOX (n58)
Venook A, et al. ASCO 2006. Abstract 3509.
70
Improved Responses with Cetuximab Added to
FOLFOX, FOLFIRI

Overall OS at 16-month FU
16.9 months without cetuximab vs not reached with
cetuximab
No unexpected toxicities
FOLFOX and FOLFIRI appear equivalent

Venook A, et al. ASCO 2006. Abstract 3509.
71
CALGB/SWOG 80405 Cetuximab, Bevacizumab, and
FOLFOX/FOLFIRI
RANDOMIZE
FOLFOX or FOLFIRI Cetuximab

First-line mCRC
Planned accrual 2300

FOLFOX or FOLFIRI Cetuximab Bevacizumab
FOLFOX or FOLFIRI Bevacizumab
Physician-selected chemotherapy. Stratification
based on chemotherapy, prior adjuvant
chemotherapy, prior pelvic RT. Study Chairs,
Alan P. Venook MD, University of California, San
Francisco and Charles D. Blanke, MD, FACP, Oregon
Health and Science University.
72
Unanswered Questions About Cetuximab

Must it be used with irinotecan?
First-line or refractory disease?
Adjuvant therapy?
Combinations of HER-1/HER-2 inhibitors?

73
Newest mAbs Are Fully Human
Matuzumab
Panitumumab
Cetuximab
Chimeric 34 mouse
Humanized 10 mouse
100 human
100 mouse
Developments in Hybridoma Technology
74
Possible Advantages of Fully Humanized Antibody

May reduce likelihood of generating antibodies
against therapeutic antibody
Could maximize efficacy over long treatment
period
May reduce risk of developing infusion reactions

75
Panitumumab Proposed Mechanism of Action
Not FDA approved for the treatment of
CRC. Weiner LM, et al. ASCO 2005. Poster
presentation available at http//www.abgenix.com/d
ocuments/ASCO20200520Weiner20Poster20FINAL.pdf
. Accessed 8/24/05.
76
Panitumumab Human Anti-EGFRPhase II Study

Patients with mCRC failing multiple standard
chemotherapy regimens (N148)
Prior treatment failure
Fluoropyrimidine leucovorin
Irinotecan, oxaliplatin, or both
EGFR overexpression by IHC required
Patients with brain metastases ineligible
2.5 mg/kg IV panitumumab given weekly over 1-h
infusion in 8-wk cycles

Malik I, et al. ASCO 2005. Abstract 3520.
77
Panitumumab Activity

Results comparable to cetuximab
PR, 9
SD, 29
Median PFS, 13.6 weeks (95 CI, 8.3-16.1 weeks)
Median OS, 37.6 weeks (95 CI, 25.6-42.4 weeks)
Responses observed in patients with up to 4 prior
regimens
Response rates not affected by EGFR expression

Malik I, et al. ASCO 2005. Abstract 3520.
78
Panitumumab Phase II Monotherapy Safety

Skin toxicity in 95 of patients
Grade 3 AEs
Skin toxicity, 7
Fatigue, 3
Vomiting, nausea, dyspnea, diarrhea
1 each
One infusion-related grade 3 event on second
infusion
Grade 4 pulmonary embolism, 1
No HAHA in 107 patients tested at baseline,
postbaseline

Malik I, et al. ASCO 2005. Abstract 3520.
79
Panitumumab Active in EGFR Low/Negative mCRC

Phase II study of treatment-refractory patients
with mCRC with low or negative EGFR expression1
88 patients enrolled to receive 6 mg/kg
panitumumab q2 wk
Interim analysis of efficacy (n23), safety
(n80)
Week 16 PR13 (EGFR-neg vs low, 18 vs 8)
Skin toxicity, 93 (15 grade 3)
Infusion reactions, 5 (grade 3, 1)
Similar findings in interim analysis of 39
patients with EGFR expression gt10 (8 PR rate,
21 SD)2

1. Hecht JR, et al. ASCO 2006. Abstract 3547. 2.
Berlin J, et al. ASCO 2006. Abstract 3548.
80
Phase III Study Panitumumab vs Best Supportive
Care
RANDOMIZE
Panitumumab (6 mg/kg q2 wk) BSC (n231)
PD

N463
Patients third-line mCRC
EGFR expression required

Stratification based on ECOG score, geographic
region
Optional Panitumumab Crossover study
Best Supportive Care (n232)
PD
Peeters M, et al. AACR 2006. Abstract CP-1.
81
Panitumumab Improves PFS Over Best Supportive Care

PFS significantly longer with panitumumab vs BSC
Hazard ratio, 0.54 (95 CI, 0.44-0.66
Plt0.000000001)
No correlation between EGFR expression, responses
No grade 3/4 infusion reactions

Plt0.0001 Peeters M, et al. AACR 2006. Abstract
CP-1.
82
Panitumumab vs Best Supportive Care Results

Crossover study
1 CR, 9 PR, 32 SD
At interim analysis (n250), OS equivalent
OS after censoring BSC patients who responded in
crossover
HR with panitumumab0.78 (95 CI, 0.61-1.01)
Severity of skin toxicity correlated with overall
survival
Grade 2-4 vs grade 1, HR0.61 (95 CI, 0.40-0.95
P0.0278)
No anti-panitumumab Abs detected after treatment
in 185 patients tested

Peeters M, et al. AACR 2006. Abstract CP-1.
83
Panitumumab vs Best Supportive Care in mCRC
Safety
Treated with IV magnesium replacement 2
developed 2o hypercalcemia. Peeters M, et al.
AACR 2006. Abstract CP-1.
84
PACCE Panitumumab Advanced CRC Evaluation Study
RANDOMIZE
Panitumumab Oxaliplatin- or irinotecan-based
chemotherapy bevacizumab (q2 wk)

First-line mCRC
No CNS metastases
No CV risk factors

Oxaliplatin- or irinotecan-based chemotherapy
bevacizumab (q2 wk)
Trial supported by Amgen, Inc.
85
Small Molecule Inhibitors Gefitinib, Erlotinib,
PTK/ZK

Considered inactive as single agent in refractory
patients
Small phase II data of standard chemotherapy with
erlotinib or gefitinib suggest possible
incremental benefit vs historical control
GERCOR trial in Europe testing FOLFOX/bevacizumab
vs XELOX/bevacizumab /- erlotinib in first line
(2x2 design)
Large phase III trial showed no improvement
adding PTK/ZK to FOLFOX4 in first-line mCRC

Kuo T, et al. J Clin Oncol. 2005235613-5619
Meyerhardt JA, et al. J Clin Oncol.
2006241892-1897 Hecht JR, et al. ASCO 2005.
Abstract 3.
86
NCCN Guidelines Advanced/mCRC
Recommendations for Patients with Good Tolerance
to Intensive Therapy
NCCN Guidelines. Version 2.2006 April 2006.
87
NCCN Guidelines Advanced/mCRC
Recommendations for Patients with Poor Tolerance
to Intensive Therapy
NCCN Guidelines. Version 2.2006 April 2006.
88
Special Consideration for Liver Metastases

Liver is the most common site of distal
metastases
25 of patients with liver metastases have no
other metastases, can be treated with regional
therapy
Regional therapies being investigated
Cryosurgery
Hepatic artery infusion of floxuridine (FUDR)
Radiofrequency ablation
Systemic chemotherapy often best option for
metastases beyond the liver

Yoon SS, Tanabe KK. Oncologist. 19994197-208.
89
Survival after Primary or Secondary Resection of
Liver Metastases
1
Resectable (N425) Initially nonresectable
(N95)
0.9
0.8
0.7
54
0.6
0.5
Proportion surviving
34
0.4
27
50
0.3
34
0.2
29
19
0.1
0
10
8
6
4
2
0
Survival time (years)
Topham C, Adam R. Semin Oncol. 2002293.
90
LiverMetSurvey Prognostic Factors in Liver
Metastases

International internet registry evaluating
prognostic factors
In 2,122 evaluable patients
5 y OS42
10 y OS26
Independent poor prognostic factors
gt3 metastases (Plt0.0001)
Bilateral metastases (P0.0002)
Largest metastasis gt5 cm (P0.03)
Preoperative chemotherapy improved survival only
in patients with gt5 metastases

Adam R, et al. ASCO 2006. Abstract 3521.
91
Adjuvant Treatment of Colon Cancer
92
Adjuvant Treatment According to Stage

Stage I
No adjuvant treatment
Stage II
Treatment controversial
Stage III
Consensus for treatment

93
Recent Advances in Adjuvant Therapy

FOLFOX4 recommended for early stage colon cancer1
Irinotecan not beneficial in multiple trials
Capecitabine active as single agent2
Continuous infusion of 5-FU less toxic, as
effective as bolus FU or FU/LV3
Current studies investigating targeted agents
Cetuximab, bevacizumab

1. Andre T, et al. N Engl J Med.
20043502343-2351. 2. Twelves C, et al. N Engl J
Med. 2005352(26)2696-2704. 3. Meta-analysis
Group in Cancer. J Clin Oncol. 199816301-308.
94
MOSAIC FOLFOX4 vs LV5FU2
RANDOMIZE
FOLFOX4 oxaliplatin, leucovorin, fluorouracil
(bolus infusion) (n1123)
N2246 Patients with resected stage II/III colon
cancer
LV5FU2 leucovorin, fluorouracil (bolus
infusion) (n1123)
Andre T, et al. N Engl J Med. 20043502343-2351.
95
Superior DFS with FOLFOX4 vs LV5FU2

Stage III patients
Significant 25 DFS risk reduction at 4.7 y
Stage II patients
No significant DFS risk reduction at 4.7 y

Plt0.001. 1. Andre T, et al. N Engl J Med.
20043502343-2351. 2. de Gramont A, et al. ASCO
2005. Abstract 3501.
96
Toxicity with FOLFOX4 vs LV5FU2

All-cause mortality, 0.5 each arm

Late recovery from sensory neuropathy was
observed. de Gramont A, et al. ASCO 2005.
Abstract 3501.
97
MOSAIC FOLFOX4 vs LV5FU2

In 2,246 patients with resected stage II/III
colon cancer, FOLFOX provided 24 relative risk
reduction in 4-y DFS
More neutropenia, sensory neuropathy with FOLFOX4
Late recovery from neuropathy observed
All-cause mortality equivalent between arms (0.5)

98
Adjuvant Therapy for Stage II Disease Where Do
We Stand?

FDA approved FOLFOX4 for stage III disease only
Main limitation for stage II clinical trials
Absolute benefit expected is about half the
benefit in stage III
Twice as many patients are needed
Available studies not powered to detect a
statistically significant benefit in this
subgroup of patients

99
Adjuvant Chemotherapy in Stage II Disease

Important to discuss potential risks/benefit with
patient
Factors to consider
Number of LN analyzed
Poor prognostic features
Comorbidities
Anticipated life expectancy
Chemotherapy not appropriate for all patients

100
Irinotecan Negative in Adjuvant Setting
1. Saltz L, et al. ASCO 2004. Abstract 3500. 2.
Van Cutsem E, et al. ASCO 2005. Abstract 8. 3.
Ychou M, et al. ASCO 2005. Abstract 3502.
101
NSABP C-07 FLOX vs 5-FU/LV
RANDOMIZE
FLOX Weekly LV-modulated 5-FU/LV
Oxaliplatin (n1200)
N2407 Patients with stage II/III colon cancer
FULV Weekly LV-modulated bolus 5-FU/LV (n1207)
Wolmark N, et al. ASCO 2005. Abstract 3500.
102
Superior DFS with FLOX vs FULV
1
0.9
0.8
DFS probability
0.7
Plt0.004 HR 0.79 95 CI, 0.67-0.93
0.6
0.5
0
1
2
3
4
Wolmark N, et al. ASCO 2005. Abstract 3500.
103
Toxicity with FLOX vs FULV

Symptoms more often reported by patients on FLOX
vs FULV 18 mo after treatment (n395)
Ringing in ears (OR, 2.4) foot discomfort (OR,
4.4) foot numbness/tingling (OR, 6.0) hand/foot
pain in cold (OR, 2.9)

Due to bowel wall thickening. Wolmark N, et al.
ASCO 2005. Abstract 3500. Land SR, et al. ASCO
2006. Abstract 3564.
104
X-ACT Capecitabine vs 5-FU/LV
24 wk
RANDOMIZE
Oral capecitabine (1250 mg/m2 bid on d1-14 q21
d) (n1004)
N1987 Patients with resected stage III colon
cancer
Bolus 5-FU leucovorin (Mayo Clinic
Regimen) (n983)
Twelves C, et al. N Engl J Med.
20053522696-2704.
105
Capecitabine As Effective As Monthly Bolus of
5-FU/LV
1.0 0.8 0.6 0.4
3-year DFS Capecitabine (n1
004) 64.2 5-FU/LV (n983) 60.6
Estimated probability
HR0.87 (95 CI, 0.75-1.00)P0.0528
0 1 2 3 4 5 6
Years
Twelves C, et al. N Engl J Med.
2005352(26)2696-2704.
106
Improved Safety with Capecitabine vs Monthly
Bolus 5-FU/LV
Treatment-related Grade 3/4 AEs
100 80 60 40 20 0
Capecitabine (n993) Bolus 5-FU/LV (n974)
Patients ()

Diarrhea Stomatitis Hand-foot Neutropenia
Nausea/ Alopecia syndrome vomiting
Plt0.001. Cassidy J, et al. ASCO 2004. Abstract
219.
107
X-ACT Study Conclusions

Capecitabine at least equivalent to IV 5-FU/LV
Fewer adverse events with capecitabine
Dose used (1250 mg/m2 bid x 14 d) is higher than
most oncologists would use in patients with
advanced disease

Twelves C, et al. N Engl J Med.
2005352(26)2696-2704. Cassidy J, et al. ASCO
2004. Abstract 219.
108
NSABP C-08 mFOLFOX6 Bevacizumab
RANDOMIZE
Bevacizumab q14 d for 6 mo (in absence of PD)
mFOLFOX6 Bevacizumab q14 d for 12 courses

Patients with resected stage II/III colon cancer
Target enrollment, 2632

mFOLFOX6 q14 d for 12 courses
Trial opened Sept 2004.
Study Chair, Carmen J. Allegra, MD, Network for
Medical Communication and Research.
109
AVANT Trial FOLFOX vs FOLFOX/BEV vs XELOX/BEV
Temporarily Suspended due to Deaths on
XELOX/Bevacizumab Arm Independent DSMB
Recommended Resuming Recruitment in May 2006
RANDOMIZE
FOLFOX4

Patients with stage II/III colon cancer
Target enrollment, 3450

FOLFOX4 Bevacizumab
XELOX Bevacizumab
de Gramont A. Hôpital Saint- Antoine, Paris,
France.
110
N0147 Adjuvant Cetuximab
RANDOMIZE
FOLFOX4 Cetuximab

Patients with resected stage III colon cancer
Target enrollment, 2300

(FOLFOX then FOLFIRI) Cetuximab
FOLFIRI Cetuximab
Study by NCCTG/NCI/ECOG. Principal Investigator,
Frank Sinicrope, MD, Mayo Clinic.
111
NCCN Guidelines for Adjuvant Therapy

For stage III patients
6 months of 5-FU/LV, capecitabine, or
5-FU/LV/oxaliplatin (FLOX, FOLFOX4, mFOLFOX6)
Same recommendation for stage II patients with no
high-risk features
For high-risk stage II patients
Consider same regimens
Consider radiation therapy for patients with T4
penetration to a fixed structure

Category 2B (nonuniform consensus). NCCN
Guidelines. Version 2.2006 April 2006.
112
Preoperative vs Postoperative ChemoRT in Rectal
Cancer

823 patients received preoperative or
postoperative chemoradiotherapy
Less toxicity with preoperative CMT no survival
difference

Sauer R, et al. N Engl J Med. 20043511731-1740.
113
Long-term Outcomes after CMT Followed by TME for
Rectal Cancer

297 consecutive patients with locally advanced
rectal cancer received preoperative CMT followed
by TME
Estimated 10-year OS, 58
Estimated 10-year RFS, 62
OS significantly improved among patients with
gt95 pathologic response

Guillem JG, et al. Ann Surg. 2005241829-838.
114
Moving Forward Topics of Ongoing Research in CRC

Determine best setting for different agents
Optimize sequence of therapies
Evaluate new agents and regional therapeutic
approaches
Define molecular mechanisms of CRC to identify
Novel ways of approaching known targets
New therapeutic targets
Patients most likely to benefit from targeted
therapies
Methods of monitoring response to therapy

115
Improving Outcomes in Colorectal Cancer
116
Treatment Choices and Challenges

Incorporate discussions across disciplines
Improve early detection and appropriate adjuvant
therapy
Further define predictors of response
Define lengths of treatment
Ensure on-time delivery and full, planned dose of
chemotherapy to optimize outcomes
Can we return to therapy previously used?
Cost/benefit analyses must continue
Continue development of newer agents

117
Factors beyond Treatment Selection Are Central to
Outcomes

Other factors in treatment have significant
impact on clinical outcomes
Quality of care
Management of side effects
Patient education, involvement, and communication
Effective therapies given in the proper disease
setting with a high quality of care will produce
the best clinical outcomes

118
Quality of Cancer Care Is an Important Component
of Treatment

Many patients believe they are receiving
suboptimal care
Benefits of measuring quality of care
Focuses us to improve quality
Identifies areas that need improving
Quality Oncology Practice Initiative (QOPI)
Coordinated by ASCO
Promotes self-examination, improvement
Every 6 months measures developed by oncologists
are collected
Practice identities concealed, data entered into
database
Allows practices to compare their progress

119
Components of Quality of Cancer Care

Resources
Staff, equipment
Clinical outcomes
Are results meeting expected targets?
Process
Proper timing, use of screenings, prescribing
medications, vaccinations

120
Patient Issues in Colorectal Cancer

Symptom management key to success of therapy
Careful monitoring allows early intervention
Assess AE risk at baseline
Comorbidities, current medications, risk of
bleeding/clotting, family history, etc
Educate patients on importance of monitoring for
symptoms, complications
Example blood pressure monitoring

121
Delivered Chemotherapy Dose Intensity and
Treatment Outcomes

Positive relationship between dose intensity,
tumor response rate demonstrated in many common
cancers, including CRC
Achieving improved clinical outcomes may depend
on delivering chemotherapy above a certain
threshold of dose intensity

Chu E, DeVita VT Jr. In DeVita VT, et al.
Cancer Principles Practice of Oncology.
2001289-306.
122
Ways to Enhance Chemotherapy Dose Delivery

Effective tools for evaluation important
Develop performance improvement tool(s) to help
track current practices in chemotherapy
administration
Adequate and proactive risk assessment
Active reviews
Study rate of toxicities and determine if
preventive methods are being appropriately used
Education
Educate personnel, including physicians, about
RDI
Advocacy
Use RN advocate to keep patients on track
Proactive attitude and prevention
Use preventive measures to avoid cancellations,
reduce complications and enhance RDI

123
Managing Side Effects in Colorectal Cancer
124
Fatigue Affects Most Cancer Patients

Physiologic predisposing factor/etiologies
Underlying disease
Treatment (anemia, infection, malnutrition, etc)
Sleep disorders
Immobility, lack of exercise
Chronic pain
Use of centrally acting drugs
Psychosocial factors

125
Patient-reported Areas Negatively Affected by
Fatigue
Ability to work
61
Physical well-being
60
Ability to enjoy lifein the moment
57
Emotional well-being
51
Intimacy with partner
44
Ability to take care of family
42
Relationships with family and friends
38
Concerns about mortality and survival
33
0
10
20
30
40
50
60
70
Patients ()
Vogelzang NJ, et al. Semin Hematol. 199734(suppl
2)4-12.
126
Cancer-related Fatigue an Important Issue

Patients reported that fatigue had greater impact
on daily life than pain
80 of oncologists considered fatigue to be
undertreated or overlooked
50 of patients discussed treatment options for
fatigue with oncologists
27 of oncologists recommended any treatment
Treatments for fatigue generally successful when
used

Vogelzang NJ, et al. Semin Hematol. 199734(suppl
2)4-12.
127
Managing Fatigue in Patients with Colorectal
Cancer

Patient education is key
Correct potential etiologies if possible
Treat anemia, sleep disorders, etc
Antidepressants for fatigue-associated major
depression
Pharmacologic treatments
Psychostimulants, low-dose corticosteroids
Nonpharmacologic strategies
Exercise, stress management, nutrition, activity
modification

Portenoy RK, Itri LM. Oncologist. 199941-10.
128
Anemia Highly Prevalent in Colorectal Cancer

Prevalence increases from 44 to 63 with
radiation

100
90
80
70
61.49
60
58.25
Percentage of cancer patients with anemia
507
50
49.66
40
39.511
32.48
30
2910
25.94
22.43
20.512
20
122
10
7.91
0
Lung
Prostate
Ovarian
Colon
Head and
Larynx
neck
Adapted from http//www.anemia.org/professionals/r
esources/slides/cancer.ppt388,19,Slide 19. 1.
Rassam JW, et al. Thorax. 19753086-90 2. Song
SZ, et al. Chin Med J (Engl). 198710097-102 3.
Dunphy EP, et al. Int J Radiat Oncol Biol Phys.
1989161173-1178 4. Obermair A, et al. Oncol
Rep. 20007639-644 5. Cappell MS, et al. J
Clin Gastroenterol. 199214227-235 6. Foti CE,
et al. Am Surg. 197036129-135 7. Twine RW, et
al. J Natl Med Assoc. 198678187-192 8. Fass L,
et al. Am J Med Sci. 1966251255-259 9. Lee
WR, et al. Int J Radiat Oncol Biol Phys.
1998421069-1075 10. Dubray B, et al.
Radiology. 1996201553-558 11. Von Knorring,
et al. Scand J Urol Nephrol. 198115279-283 12.
Grant KL. P and T. 199318191.
129
Negative Consequences of Anemia in CRC

Fatigue
Decreased quality of life
Increased mortality
Decreased treatment efficacy

130
NCCN Clinical Practice Guidelines Algorithm for
Cancer and Treatment-related Anemia
Asymptomatic (risk factors)
Asymptomatic (no risk factors)
Symptomatic
Transfuse as indicated and/or consider
erythropoietic therapy
Observation and periodic re-evaluation
Consider erythropoietic therapy
Conduct iron studies (serum iron, total
iron-binding capacity, serum ferritin)
Epoetin alfa
Darbepoetin alfa
Hb 10-11 g/dL consider erythropoietic therapy
Hblt10 g/dL strongly consider erythropoietic
therapy NCCN. Clinical Practice Guidelines in
Oncology v.2.2006-Cancer and Treatment-related
Anemia Available at http//www.nccn.org/physician
_gls/f_guidelines.html. Accessed June 24, 2006.
131
Darbepoetin alfa in CIA in GI Cancers

2 studies enrolled 671 patients with GI cancers
and anemia
Study 2 regimen effective with lower mean weekly
dose

Without imputation. Blayney D, et al. ASCO GI
2005. Abstract 251.
132
Every-3-Week Darbepoetin alfa Noninferior to
Weekly Dosing

Double-blind, randomized, active-control phase
III trial of 705 patients (16 CRC) with anemia
receiving chemotherapy
Study compared two DA doses (N705)
Weekly (2.25 mg/kg) or q3 wk (500 mg) for 15
weeks
q3 wk dose noninferior to weekly dose
Fewer transfusions with q3 wk (unadjusted, 23 vs
30)
Target Hb with q3 wk vs weekly
84 vs 77
Safety comparable

Canon JL, et al. J Natl Cancer Inst.
200698273-284.
133
2006 NCCN Anemia Guidelines Erythropoietic
Therapy Options
Epoetin alfa 150 U/kg tiw
Increase to 300 U/kg tiw
or Epoetin alfa 40,000 U q wk
Increase to 60,000 U q wk
or Darbepoetin alfa 2.25 µg/kg q wk
Increase to 4.5 µg/kg q wk
or Darbepoetin alfa 500 µg q3 wk
Decrease to 300 µg/kg q3 wk Darbepoetin
alfa 3 µg/kg q2 wk Increase to 5 µg/kg q2 wk
or Darbepoetin alfa 200 µg q2 wk Increase to
300 µg q2 wk
Package Insert Dosing
Commonly Used Regimens
Boccia R, et al. Oncologist. 200611(4)409-417.
NCCN. Clinical Practice Guidelines in Oncology
v.2.2006-Cancer and Treatment-related Anemia.
Available at http//www.nccn.org/physician_gls/f_
guidelines.html. Accessed May 15, 2006.
134
Treatment-specific Side Effects in Colorectal
Cancer
135
Managing Irinotecan Side Effects

Early diarrhea, other cholinergic symptoms
Prevent or treat with atropine (0.25-1 mg IV or
SC)
Late diarrhea
Treat promptly with loperamide
Fluid, electrolyte replacement
Antibiotics for ileus, fever, severe neutropenia
Delay chemotherapy until bowel function returns
to pretreatment level for 24 hours with no
anti-diarrhea medication
Grade 2-4 late diarrhea ? decrease irinotecan dose

Camptosar (irinotecan) Prescribing Information.
New York, NY Pfizer, Inc. July 2005
136
Managing Irinotecan Side Effects (cont.)

Manage neutropenic complications with antibiotics
Temporarily omit irinotecan during cycle if
Neutropenic fever
ANC lt1000/mm3
After ANC gt1000/mm3, reduce irinotecan dose
Consider CSF if neutropenia significant

Camptosar (irinotecan) Prescribing Information.
New York, NY Pfizer, Inc. July 2005.
137
NCI Recommendations for Managing IFL-induced
Diarrhea
Benson AL, et al. J Clin Oncol. 2004222918-2926.
138
Managing Oxaliplatin Side Effects

Common
Acute neurotoxicity (in 1st 2 wk of therapy)
Distal paresthesias (numbness, tingling) or
dysesthesias (pain) often triggered by cold
Reversible by warming hands
Rare (lt1)
Pharyngolaryngeal dysesthesia
Educate patients to breathe in warm air, drink
warm fluids
Chronic neurotoxicity (cumulative- after several
cycles)
Reversible- usually gone within 1 year

139
Managing Oxaliplatin Side Effects (cont.)

Calcium gluconate (1 g) and magnesium sulfate (1
g) 15 min before, after oxaliplatin
Small retrospective study showed substantial
reduction in any neuropathy1
Increase duration of infusion (up to 6 hours)
Oral calcium and magnesium (anecdotal)

1. Gamelin E, et al. ASCO 2002. Abstract 624.
140
Xaliproden Reduces Oxaliplatin-related Neuropathy

18-20 of patients on oxaliplatin develop grade
3/4 PSN
Xaliproden
An oral neurotrophic agent
Double-blind, randomized, controlled, phase III
trial
649 patients with first-line mCRC received
FOLFOX4 xaliproden or placebo
Xaliproden reduced grade 3/4 PSN by 39
(P0.0203)
No effect on FOLFOX4 efficacy

Cassidy J, et al. 2006 ASCO Gastrointestinal
Cancers Symposium. Abstract 229.
141
Managing Capecitabine Side Effects

Patient education key for this home-based therapy
Capecitabine can produce 5-FU-like side effects
Most symptoms less common than with IV 5-FU
Only hand-foot syndrome more common
Treatment modification only proven relief
Temporary interruption, dose modification will
likely resolve symptoms without adversely
affecting outcomes

Marse H, et al. Eur J Oncol Nurs.
20048(suppl1)S16-30.
142
Managing Bevacizumab Side Effects

Hypertension common with bevacizumab
Suggest lifestyle modifications
New or additional hypertensive therapy may be
needed
Monitor blood pressure at least every 2-3 wk
More frequently in those who develop hypertension
Monitor patients for bleeding

143
Managing Bevacizumab Side Effects (cont.)

Assess for signs of potential thrombosis
Initiate treatment promptly if thromboembolic
event occurs
Infusion-related symptoms
Usually mild and self-limited
Most often occur during first few infusions
If symptoms develop
Stop infusion until symptoms improve
Use medications according to protocol
(antihistamines, corticosteroids, acetaminophen,
etc)

144
Treating EGFR-associated Rash
Segaert S, Van Cutsem E. Ann Oncol.
2005161425-1433.
145
Rash Management Recommendations for Patients

Hydrating measures
Bath oils instead of gel/soap
Wash in tepid water
Emollients
Limit sun exposure use sunscreens
Avoid tight shoes to prevent paronychia
Explain to patient link between rash, response
rate

Segaert S, Van Cutsem E. Ann Oncol.
2005161425-1433.
146
Cetuximab Infusion Reactions

3 of patients have severe reactions 90 at
first infusion
Administer prophylactic H1 antagonist prior to
infusion
Grade 1/2
Permanently reduce infusion rate by 50
Grade 3/4
Immediately, permanently discontinue cetuximab
Management strategies
Monitor patient vigilantly
Have readily available resources
Initiate protocols per institution or practice

Erbitux (cetuximab) Prescribing Information.
ImClone Systems and BMS, Inc. March 2006.
147
Appendix

Other GI Cancers

148
Pancreatic Cancer
149
Current State of Pancreatic Cancer

Fourth leading cause of cancer-related death in
US
1-y survival lt20 5-y survival lt5
Surgery only potential curative option only 15
of patients are candidates
Systemic therapy with gemcitabine standard
therapy since 1997
Continued investigations into combination therapy

Jemal A, et al. CA Cancer J Clin.
20055510-30. Lillemoe KD. Ann Surg.
1995221133-148.
150
Agents Evaluated with Gemcitabine Showing No
Overall Survival Benefit
1. Riess H, et al. ASCO 2005. Abstract 4009 2.
Herrmann R, et al. ASCO 2005. Abstract 4010 3.
Rocha Lima CM, et al. J Clin Oncol. Abstract
3776 4. Heinmann V, et al. ASCO 2003. Abstract
1003 5. OReilly E, et al. ASCO 2004. Abstract
4006 6. Richards DA, et al. ASCO 2004. Abstract
4007 7. Louvet C, et al. ASCO 2004. Abstract
4008.
151
Gemcitabine Capecitabine in Pancreatic Cancer
RANDOMIZE
Gemcitabine Capecitabine Gemcitabine 1000 mg/m2
weekly x 3 q4 wk Capecitabine 1660 mg/m2/d for 21
days then 7 days rest (n267)
N553 Patients with previously untreated
advanced/ metastatic pancreatic cancer
Gemcitabine (1000 mg/m2 weekly x 7 q8 wk then 1
wk rest thereafter weekly x 3 q4 wk) (n266)
Cunningham D, et al. European Cancer Conference
(ECCO) 2005. Abstract PS11.
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Superior Survival with Gemcitabine Capecitabine
in Pancreatic Cancer

20 improvement in overall survival with
combination

P0.026. Cunningham D, et al. European Cancer
Conference (ECCO) 2005. Abstract PS11.
153
Gemcitabine Erlotinib Approved for Advanced
Pancreatic Cancer

Based on phase III trial of 569 patients
Addition of erlotinib to gemcitabine
significantly improved survival vs gemcitabine
alone
Superior OS ? HR, 0.81 (95 CI, 0.67-0.97
P0.025)
Longer 1-year survival (24 vs 17)
Longer PFS ? HR, 0.76 (P0.003)
Incidence of grade 3/4 toxicity equivalent
between groups

Moore MJ, et al. J Clin Oncol. 20052316s.
Abstract 1.
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Gem Platin A

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